The Wilms’ Tumor Suppressor Gene ( wt1 ) Product Regulates Dax-1 Gene Expression during Gonadal Differentiation

Author:

Kim Jungho1,Prawitt Dirk2,Bardeesy Nabeel1,Torban Elena3,Vicaner Caroline3,Goodyer Paul3,Zabel Bernard2,Pelletier Jerry14

Affiliation:

1. Department of Biochemistry,1

2. Department of Pediatrics, University of Mainz, D-55101 Mainz, Germany2

3. Department of Pediatrics, Experimental Medicine, 3 McGill University, Montreal, Quebec, Canada, and

4. McGill Cancer Center, 4 and

Abstract

ABSTRACT Gonadal differentiation is dependent upon a molecular cascade responsible for ovarian or testicular development from the bipotential gonadal ridge. Genetic analysis has implicated a number of gene products essential for this process, which include Sry, WT1, SF-1, and DAX-1. We have sought to better define the role of WT1 in this process by identifying downstream targets of WT1 during normal gonadal development. We have noticed that in the developing murine gonadal ridge, wt1 expression precedes expression of Dax-1 , a nuclear receptor gene. We document here that the spatial distribution profiles of both proteins in the developing gonad overlap. We also demonstrate that WT1 can activate the Dax-1 promoter. Footprinting analysis, transient transfections, promoter mutagenesis, and mobility shift assays suggest that WT1 regulates Dax-1 via GC-rich binding sites found upstream of the Dax-1 TATA box. We show that two WT1-interacting proteins, the product of a Denys-Drash syndrome allele of wt1 and prostate apoptosis response-4 protein, inhibit WT1-mediated transactivation of Dax-1 . In addition, we demonstrate that WT1 can activate the endogenous Dax-1 promoter. Our results indicate that the WT1–DAX-1 pathway is an early event in the process of mammalian sex determination.

Publisher

American Society for Microbiology

Subject

Cell Biology,Molecular Biology

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